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Elevated H3K27ac in aged skeletal muscle leads to increase in extracellular matrix and fibrogenic conversion of muscle satellite cells

机译:老年骨骼肌中H3K27ac升高导致细胞外基质增加以及肌肉卫星细胞的纤维化转化

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摘要

Epigenetic alterations occur in various cells and tissues during aging, but it is not known if such alterations are also associated with aging in skeletal muscle. Here, we examined the changes of a panel of histone modifications and found H3K27ac (an active enhancer mark) is markedly increased in aged human skeletal muscle tissues. Further analyses uncovered that the H3K27ac increase and enhancer activation are associated with the up‐regulation of extracellular matrix (ECM) genes; this may result in alteration of the niche environment for skeletal muscle stem cells, also called satellite cells (SCs), which causes decreased myogenic potential and fibrogenic conversion of SCs. In mice, treatment of aging muscles with JQ1, an inhibitor of enhancer activation, inhibited the ECM up‐regulation and fibrogenic conversion of SCs and restored their myogenic differentiation potential. Altogether, our findings not only uncovered a novel aspect of skeletal muscle aging that is associated with enhancer remodeling but also implicated JQ1 as a potential treatment approach for restoring SC function in aging muscle.
机译:表观遗传学改变发生在衰老过程中的各种细胞和组织中,但是尚不清楚这种改变是否也与骨骼肌衰老有关。在这里,我们检查了一组组蛋白修饰的变化,发现H3K27ac(一种活性增强标记)在老年人的骨骼肌组织中显着增加。进一步的分析发现,H3K27ac的增加和增强子的激活与细胞外基质(ECM)基因的上调有关。这可能会导致骨骼肌干细胞(也称为卫星细胞(SCs))的利基环境发生变化,从而导致SC的成肌潜力降低和成纤维转化。在小鼠中,使用JQ1(增强剂激活的抑制剂)治疗衰老的肌肉,可抑制SC的ECM上调和纤维化转化,并恢复其成肌分化潜能。总而言之,我们的发现不仅揭示了与增强剂重塑有关的骨骼肌衰老的新方面,而且还暗示JQ1是恢复衰老肌肉SC功能的潜在治疗方法。

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